Horio Y, Chen A, Rice P, Roth J A, Malkinson A M, Schrump D S
Department of Thoracic and Cardiovascular Surgery, University of Texas M. D. Anderson Cancer Center, Houston 77030, USA.
Mol Carcinog. 1996 Dec;17(4):217-23. doi: 10.1002/(SICI)1098-2744(199612)17:4<217::AID-MC5>3.0.CO;2-A.
In the A/J strain of mice, urethane (ethyl carbamate) induces lung hyperplasia, adenoma, and adenocarcinoma in a time-dependent manner. These distinct morphological stages may correlate with sequential molecular genetic changes in this mouse model. To test this hypothesis, we investigated the presence of mutations involving Ki-ras and p53 in urethane-induced lung lesions in A/J mice at early and late stages of tumorigenesis. We precisely microdissected 40 lung lesions from paraffin-embedded sections. Ki-ras mutations around codon 61 and p53 mutations in exons 5-8 were identified by polymerase chain reaction-single-strand conformation polymorphism and DNA sequencing techniques. In 29 early-stage lung lesions classified as hyperplasias (seven) or adenomas (22), we observed 19 Ki-ras mutations (66%), including three silent mutations and one double mutation at different codons, and one silent p53 mutation (3.5%). In 11 late-stage adenomas, we identified nine activating Ki-ras mutations (82%) and four missense p53 mutations (36%). These results indicate that Ki-ras mutations arise early, whereas p53 mutations occur relatively late during the benign stages of urethane-induced lung carcinogenesis in A/J mice.
在A/J品系小鼠中,氨基甲酸乙酯(尿烷)以时间依赖性方式诱导肺增生、腺瘤和腺癌。在这个小鼠模型中,这些不同的形态学阶段可能与连续的分子遗传学变化相关。为了验证这一假设,我们研究了在A/J小鼠氨基甲酸乙酯诱导的肺损伤发生肿瘤的早期和晚期阶段,是否存在涉及Ki-ras和p53的突变。我们从石蜡包埋切片中精确地显微切割了40个肺损伤组织。通过聚合酶链反应-单链构象多态性和DNA测序技术鉴定了密码子61周围的Ki-ras突变以及外显子5-8中的p53突变。在29个早期肺损伤组织中,其中7个为增生性病变,22个为腺瘤,我们观察到19个Ki-ras突变(66%),包括3个沉默突变和1个不同密码子处的双重突变,以及1个沉默的p53突变(3.5%)。在11个晚期腺瘤中,我们鉴定出9个激活的Ki-ras突变(82%)和4个错义p53突变(36%)。这些结果表明,在A/J小鼠氨基甲酸乙酯诱导的肺癌发生的良性阶段,Ki-ras突变出现较早,而p53突变出现相对较晚。
